Sera from patients with anti-GBM nephritis including Goodpasture syndrome show heterogenous reactivity to recombinant NC1 domain of type IV collagen {alpha} chains |
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| Authors: | Dehan, P. Weber, M. Zhang, Xu Reeders, S. T. Foidart, J.-M. Tryggvason, K. |
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| Affiliation: | 1 Biocenter Oulu and Department of Biochemistry, University of Oulu Oulu, Finland 2 Laboratory of Biology, University of Liege Liège, Belgium 3 IV Department of Medicine, University of Erlangen-Nürnberg Erlangen, Germany 4 Division of Nephrology, Brigham and Women's Hospital, Harvard Medical School Boston, MA, USA |
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| Abstract: | BACKGROUND.: Goodpasture (GP) syndrome is defined by the clinical associationof pulmonary haemorrhage with rapidly progressive glomerulonephritis.The disease is caused by pathogenic autoantibodies directedagainst type IV collagen, which is a major structural componentof glomerular basement membranes (GBM). METHODS.: The non-collagenous domains (NC1) of all six human type IV collagenchains was produced in E. coli as recombinant fusion proteinswith glutathione-S transferase. Sera from 10 patients with differenttypes of anti-GBM nephritis, including GP syndrome, were testedfor reactivity with the six proteins using immunoblotting ofdenatured and reduced proteins and ELISA without reduction. RESULTS.: All 10 sera reacted with the  3(IV) collagen chain by immunoblottingand ELISA. One serum also recognized the 2(IV) 4(IV), 5(IV)and 6(IV) chains by immunoblotting. ELISA measurements revealedreactivity of several other sera with 2(IV), 4(IV) or 6(IV)but not with 5(IV) collagen chains. No reactivity was observedwith the 1(IV) chain. CONCLUSION.: Autoantibodies in anti-GBM nephritis may not be directed onlyagainst the 3(IV) collagen chain and they frequently recognizeconformational epitopes. |
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| Keywords: | anti-GBM nephritis basement membrane IV collagen Goodpasture syndrome |
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